UMIN-CTR Clinical Trial

Public title

A Phase I/II, open-label, non-randomized, multi-center, dose escalation study of olaparib in combination with eribulin mesylate to assess the safety, tolerability, and efficacy in patients with recurrent or metastatic triple-negative-type breast cancer, who have received anthracycline and taxane agents

Acronym

A Phase I/II study of olaparib in combination with eribulin mesylate in patients with TNBC

Scientific Title

A Phase I/II, open-label, non-randomized, multi-center, dose escalation study of olaparib in combination with eribulin mesylate to assess the safety, tolerability, and efficacy in patients with recurrent or metastatic triple-negative-type breast cancer, who have received anthracycline and taxane agents

Scientific Title:Acronym

A Phase I/II study of olaparib in combination with eribulin mesylate in patients with TNBC

Region

Japan

Condition

Breast cancer

Classification by specialty

Hematology and clinical oncology

Breast surgery

Classification by malignancy

Malignancy

Genomic information

NO

Narrative objectives1

The safety, tolerability, and MTD of olaparib in combination with eribulin mesylate will be assessed, based on the incidence of dose limiting toxicity at each dose level in Phase I. The efficacy and safety of the combination will be assessed, in Phase II.

Basic objectives2

Safety,Efficacy

Basic objectives -Others

Trial characteristics_1

Exploratory

Trial characteristics_2

Developmental phase

Phase I,II

Primary outcomes

Phase I: Safety and tolerability
Phase II: Response rates

Key secondary outcomes

Study type

Interventional

Basic design

Single arm

Randomization

Non-randomized

Randomization unit

Blinding

Open -no one is blinded

Control

Uncontrolled

Stratification

Dynamic allocation

Institution consideration

Blocking

Concealment

No. of arms

1

Purpose of intervention

Treatment

Type of intervention

Medicine

Interventions/Control_1

Eribulin mesylate administer day 1, day 8, tri-weekly interval. Olaparib administer continuously and/or intermittently according to in each cohort. The trial treatment will be continued until there is progressive disease.

Interventions/Control_2

Interventions/Control_3

Interventions/Control_4

Interventions/Control_5

Interventions/Control_6

Interventions/Control_7

Interventions/Control_8

Interventions/Control_9

Interventions/Control_10

Age-lower limit

18

years-old

<=

Age-upper limit

Not applicable

Gender

Female

Key inclusion criteria

1)Histological confirmation of invasive breast cancer
2)Unresectable clinical StageIIIB, IIIC or IV or eligible for systemic chemotherapy for recurrent breast cancer
3)Histological confirmation of breast cancer without overexpression of HER2 (0 or 1+ in immunohistocompatibility (IHC), or negative in in-situ hybridization (ISH) tests).
4)Histological confirmation of hormonal receptor-negative breast cancer (Allred score < 3 in the IHC test for estrogen receptor and progesterone receptor).
5)PS (ECOG) 0 to 1
6)A treatment history of anthracycline and taxane agents, irrespective of the type of combination or treatment order
7)Patients with the following values in their latest laboratory tests
-Neutrophil count > 1,500/mm3
-Hemoglobin > 9.0/dL
-Platelet count > 100,000/mm3
-Total bilirubin < 1.5 mg/dL
-Serum AST/ALT < 100 IU/L
-Serum creatinine < 1.2 mg/dL
-ECG Normal or minimal changes not requiring treatment and QTc interval < 450 ms
8)Recovery to grade 0 or 1 from all toxicities related to chemotherapy and radiotherapy, except for stable grade 0 to 2 sensory neuropathy and alopecia

Key exclusion criteria

1)Pregnant or breast-feeding women, or women of child bearing potential who intend to become pregnant
2)Patients who received treatment (chemotherapy or study treatment) within 1 week from the last administration or underwent treatment procedures (surgery or exposure to radiation) within the 2 weeks preceding enrollment
3)Patients with respiratory failure requiring oxygen inhalation therapy
4)Patients requiring therapeutic dosages of warfarin or related agents
5)Patients with signs or symptoms of interstitial pneumonia or pulmonary fibrosis
6)Patients who are HBs antigen-positive, HCV antibody-positive and/or HIV antibody-positive (Patients who are HBV-DNA positive and/or HCV-RNA positive are cannot be allowed)
7)Patients with serious cardiovascular disease
8)Patients with diabetes mellitus associated with poor glycemic control or receiving insulin
9)Patients with metastases to brain
10)Patients with meningeal carcinomatosis
11)Patients with gastrointestinal obstruction or the symptoms of it
12)Patients with synchronous double cancer, not including lesions equivalent to carcinoma in situ or mucosal carcinoma considered healed with topical therapy
13)Patients who have no features suggestive of MDS/AML on peripheral blood smear
14)Patients receiving the following classes of CYP3A4 inhibitors and inducers
-CYP3A4 inhibitors: Azole antifungals, Macrolide antibiotics, Protease inhibitors
-CYP3A4 inducers: Phenytoin, Rifampicin, Carbamazepine, Barbiturate derivatives
15)Patients with history of treatment with or allergy to eribulin mesylate
Patients with history of treatment with or allergy to PARP inhibitors

Target sample size

48

Name of lead principal investigator

1st name
Middle name
Last name	Kan Yonemori

Organization

National Cancer Center Hospital

Division name

Breast and Medical Oncology Division

Zip code

Address

5-1-1 Tsukiji, Chuo-ku, Tokyo104-0045, Japan

TEL

03-3542-2511

Email

Olaparib_trial_office@umin.ac.jp

Name of contact person

1st name
Middle name
Last name	Tamie Sukigara

Organization

National Cancer Center

Division name

Clinical Trial Support Office

Zip code

Address

5-1-1 Tsukiji, Chuo-ku, Tokyo104-0045, Japan

TEL

03-3547-5201

Homepage URL

Email

Olaparib_trial_office@umin.ac.jp

Institute

National Cancer Center Hospital

Institute

Department

Personal name

Organization

Japan Medical Association

Organization

Division

Category of Funding Organization

Non profit foundation

Nationality of Funding Organization

Co-sponsor

Name of secondary funder(s)

Organization

Address

Tel

Email

Secondary IDs

NO

Study ID_1

Org. issuing International ID_1

Study ID_2

Org. issuing International ID_2

IND to MHLW

Institutions

独立行政法人国立病院機構大阪医療センター（大阪府）
独立行政法人国立病院機構四国がんセンター（愛媛県）
独立行政法人国立病院機構北海道がんセンター（北海道）
地方独立行政法人神奈川県立病院機構神奈川県立がんセンター（神奈川県）
千葉県がんセンター（千葉県）
独立行政法人国立がん研究センター中央病院（東京都）

Date of disclosure of the study information

2012

Year

12

Month

10

Day

URL releasing protocol

Publication of results

Unpublished

URL related to results and publications

Number of participants that the trial has enrolled

Results

Results date posted

Results Delayed

Results Delay Reason

Date of the first journal publication of results

Baseline Characteristics

Participant flow

Adverse events

Outcome measures

Plan to share IPD

IPD sharing Plan description

Recruitment status

Completed

Date of protocol fixation

2012

Year

10

Month

05

Day

Date of IRB

Anticipated trial start date

2013

Year

01

Month

22

Day

Last follow-up date

2016

Year

09

Month

30

Day

Date of closure to data entry

Date trial data considered complete

Date analysis concluded

Other related information

Registered date

2012

Year

12

Month

06

Day

Last modified on

2018

Year

03

Month

05

Day

Link to view the page

Value
https://center6.umin.ac.jp/cgi-open-bin/ctr_e/ctr_view.cgi?recptno=R000011159